磷脂病
单酰甘油脂肪酶
生物标志物
背景(考古学)
药品
医学
毒理基因组学
药理学
毒性
生物信息学
内科学
生物
磷脂
古生物学
生物化学
内大麻素系统
遗传学
受体
基因表达
膜
基因
作者
Elizabeth Tengstrand,Gerald T. Miwa,F. Hsieh
标识
DOI:10.1517/17425251003601961
摘要
Importance to the field: Drug-induced phospholipidosis (PL) is a phospholipid storage disorder characterized by the accumulation of multi-lamellar bodies (myeloid bodies) in tissues. A major unanswered question is whether PL represents a benign adaptive response, symptom or early event in drug toxicity. The absence of a non-invasive biomarker to monitor tissue PL has made it difficult to determine the prevalence and implications of PL in the clinic. As a result, the interpretation of PL in risk assessment remains uncertain in preclinical and clinical drug development.Areas covered in this review: This review describes the rationale for bis(monoacylglycerol)phosphate (BMP) as a biomarker of PL and explores the potential links between PL and the toxicities of drugs.What the reader will gain: The similarities between the hypothesized roles of BMP in PL and Niemann-Pick type C disease are discussed. The potential implications of PL for cellular function are described in the context of drug-induced QT prolongation, myopathy and renal toxicity.Take home message: A specific species of BMP, di-docosahexaenoyl-BMP, should be investigated further as a non-invasive biomarker to monitor the onset and time course of PL and to better understand the functional consequences which could contribute to the toxicities of drugs.
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